Polymorphic DNA repair and metabolic genes: a multigenic study on gastric cancer

D Palli; Silvia POLIDORO; M D'Errico; C Saieva; S Guarrera; Calcagnile AS; F Sera; A Allione; S Gemma; I Zanna; A Filomena; E Testai; S Caini; R Moretti; Gomez-Miguel MJ; G Nesi; I Luzzi; L Ottini; G Masala; G Matullo; E Dogliotti

doi:10.1093/mutage/geq042

Polymorphic DNA repair and metabolic genes: a multigenic study on gastric cancer

D Palli
, Silvia POLIDORO
, M D'Errico
, C Saieva
, S Guarrera
, Calcagnile AS
, F Sera
, A Allione
, S Gemma
, I Zanna
, A Filomena
, E Testai
, S Caini
, R Moretti
, Gomez-Miguel MJ
, G Nesi
, I Luzzi
, L Ottini
, G Masala
, G Matullo

E Dogliotti

Dipartimento di Medicina Traslazionale

Risultato della ricerca: Contributo su rivista › Articolo in rivista › peer review

Abstract

Risk factors for gastric cancer (GC) include inter-individual variability in the inflammatory response to Helicobacter pylori infection, in the ability of detoxifying DNA reactive species and repairing DNA damage generated by oxidative stress and dietary carcinogens. To evaluate the association between polymorphic DNA repair genes and GC risk, a case-control study including 314 histologically confirmed GC patients and 548 healthy controls was conducted in a GC high-risk area in Tuscany, Italy. Polymorphic variants of base excision repair (APE1-D148E, XRCC1-R194W, XRCC1-R399Q and OGG1-S326C), nucleotide excision repair (XPC-PAT, XPA-23G>A, ERCC1-19007T>C and XPD-L751Q), recombination (XRCC3-T241M) and alkylation damage reversal (MGMT-L84F) were tested for their potential role in the development of GC by using logistic regression models. The same population was also characterised for GSTT1 and GSTM1 variant alleles to search for possible functional interactions between metabolic and DNA repair genotypes by two-way interactions using multivariate logistic models. No significant association between any single DNA repair genotype and GC risk was detected with a borderline association with the XPC-PAT homozygous genotype [odds ratio (OR) = 1.42; 95% confidence interval (CI) 0.94-2.17]. Gene-gene interaction analysis revealed combinations of unfavourable genotypes involving either multiple DNA repair polymorphisms or DNA repair and GST-specific genotypes. The combination of the XPC-PAT and the XPA variant alleles significantly increased GC risk (OR = 2.15; 95% CI 1.17-3.93, P = 0.0092). A significant interaction was also found between the APE1 wild-type genotype and either the single GSTT1 (OR = 4.90; 95% CI 2.38-10.11, P = 0.0079) or double GSTM1-GSTT1 null (OR = 7.84; 95% CI 3.19-19.22, P = 0.0169) genotypes or the XPA-mutant allele (OR = 3.56; 95% CI 1.53-8.25, P = 0.0012). These findings indicate that a complex interaction between host factors such as oxidative stress, antioxidant capacity and efficiency of multiple DNA repair pathways underlies the inter-individual variability in GC risk.

Lingua originale	Inglese
pagine (da-a)	569-575
Numero di pagine	7
Rivista	Mutagenesis
Volume	25
Numero di pubblicazione	6
DOI	https://doi.org/10.1093/mutage/geq042
Stato di pubblicazione	Pubblicato - 2010

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Keywords

DNA repair
polymorphisms
gastric cancer

Accesso al documento

10.1093/mutage/geq042

https://hdl.handle.net/11579/223163

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Palli, D., POLIDORO, S., D'Errico, M., Saieva, C., Guarrera, S., AS, C., Sera, F., Allione, A., Gemma, S., Zanna, I., Filomena, A., Testai, E., Caini, S., Moretti, R., MJ, G.-M., Nesi, G., Luzzi, I., Ottini, L., Masala, G., ... Dogliotti, E. (2010). Polymorphic DNA repair and metabolic genes: a multigenic study on gastric cancer. Mutagenesis, 25(6), 569-575. https://doi.org/10.1093/mutage/geq042

@article{538381b730ad42589da7dfa1c04bf93b,

title = "Polymorphic DNA repair and metabolic genes: a multigenic study on gastric cancer",

abstract = "Risk factors for gastric cancer (GC) include inter-individual variability in the inflammatory response to Helicobacter pylori infection, in the ability of detoxifying DNA reactive species and repairing DNA damage generated by oxidative stress and dietary carcinogens. To evaluate the association between polymorphic DNA repair genes and GC risk, a case-control study including 314 histologically confirmed GC patients and 548 healthy controls was conducted in a GC high-risk area in Tuscany, Italy. Polymorphic variants of base excision repair (APE1-D148E, XRCC1-R194W, XRCC1-R399Q and OGG1-S326C), nucleotide excision repair (XPC-PAT, XPA-23G>A, ERCC1-19007T>C and XPD-L751Q), recombination (XRCC3-T241M) and alkylation damage reversal (MGMT-L84F) were tested for their potential role in the development of GC by using logistic regression models. The same population was also characterised for GSTT1 and GSTM1 variant alleles to search for possible functional interactions between metabolic and DNA repair genotypes by two-way interactions using multivariate logistic models. No significant association between any single DNA repair genotype and GC risk was detected with a borderline association with the XPC-PAT homozygous genotype [odds ratio (OR) = 1.42; 95\% confidence interval (CI) 0.94-2.17]. Gene-gene interaction analysis revealed combinations of unfavourable genotypes involving either multiple DNA repair polymorphisms or DNA repair and GST-specific genotypes. The combination of the XPC-PAT and the XPA variant alleles significantly increased GC risk (OR = 2.15; 95\% CI 1.17-3.93, P = 0.0092). A significant interaction was also found between the APE1 wild-type genotype and either the single GSTT1 (OR = 4.90; 95\% CI 2.38-10.11, P = 0.0079) or double GSTM1-GSTT1 null (OR = 7.84; 95\% CI 3.19-19.22, P = 0.0169) genotypes or the XPA-mutant allele (OR = 3.56; 95\% CI 1.53-8.25, P = 0.0012). These findings indicate that a complex interaction between host factors such as oxidative stress, antioxidant capacity and efficiency of multiple DNA repair pathways underlies the inter-individual variability in GC risk.",

keywords = "DNA repair, polymorphisms, gastric cancer, DNA repair, polymorphisms, gastric cancer",

author = "D Palli and Silvia POLIDORO and M D'Errico and C Saieva and S Guarrera and Calcagnile AS and F Sera and A Allione and S Gemma and I Zanna and A Filomena and E Testai and S Caini and R Moretti and Gomez-Miguel MJ and G Nesi and I Luzzi and L Ottini and G Masala and G Matullo and E Dogliotti",

year = "2010",

doi = "10.1093/mutage/geq042",

language = "English",

volume = "25",

pages = "569--575",

journal = "Mutagenesis",

issn = "0267-8357",

publisher = "Oxford University Press",

number = "6",

}

Palli, D, POLIDORO, S, D'Errico, M, Saieva, C, Guarrera, S, AS, C, Sera, F, Allione, A, Gemma, S, Zanna, I, Filomena, A, Testai, E, Caini, S, Moretti, R, MJ, G-M, Nesi, G, Luzzi, I, Ottini, L, Masala, G, Matullo, G & Dogliotti, E 2010, 'Polymorphic DNA repair and metabolic genes: a multigenic study on gastric cancer', Mutagenesis, vol. 25, n. 6, pagg. 569-575. https://doi.org/10.1093/mutage/geq042

TY - JOUR

T1 - Polymorphic DNA repair and metabolic genes: a multigenic study on gastric cancer

AU - Palli, D

AU - POLIDORO, Silvia

AU - D'Errico, M

AU - Saieva, C

AU - Guarrera, S

AU - AS, Calcagnile

AU - Sera, F

AU - Allione, A

AU - Gemma, S

AU - Zanna, I

AU - Filomena, A

AU - Testai, E

AU - Caini, S

AU - Moretti, R

AU - MJ, Gomez-Miguel

AU - Nesi, G

AU - Luzzi, I

AU - Ottini, L

AU - Masala, G

AU - Matullo, G

AU - Dogliotti, E

PY - 2010

Y1 - 2010

N2 - Risk factors for gastric cancer (GC) include inter-individual variability in the inflammatory response to Helicobacter pylori infection, in the ability of detoxifying DNA reactive species and repairing DNA damage generated by oxidative stress and dietary carcinogens. To evaluate the association between polymorphic DNA repair genes and GC risk, a case-control study including 314 histologically confirmed GC patients and 548 healthy controls was conducted in a GC high-risk area in Tuscany, Italy. Polymorphic variants of base excision repair (APE1-D148E, XRCC1-R194W, XRCC1-R399Q and OGG1-S326C), nucleotide excision repair (XPC-PAT, XPA-23G>A, ERCC1-19007T>C and XPD-L751Q), recombination (XRCC3-T241M) and alkylation damage reversal (MGMT-L84F) were tested for their potential role in the development of GC by using logistic regression models. The same population was also characterised for GSTT1 and GSTM1 variant alleles to search for possible functional interactions between metabolic and DNA repair genotypes by two-way interactions using multivariate logistic models. No significant association between any single DNA repair genotype and GC risk was detected with a borderline association with the XPC-PAT homozygous genotype [odds ratio (OR) = 1.42; 95% confidence interval (CI) 0.94-2.17]. Gene-gene interaction analysis revealed combinations of unfavourable genotypes involving either multiple DNA repair polymorphisms or DNA repair and GST-specific genotypes. The combination of the XPC-PAT and the XPA variant alleles significantly increased GC risk (OR = 2.15; 95% CI 1.17-3.93, P = 0.0092). A significant interaction was also found between the APE1 wild-type genotype and either the single GSTT1 (OR = 4.90; 95% CI 2.38-10.11, P = 0.0079) or double GSTM1-GSTT1 null (OR = 7.84; 95% CI 3.19-19.22, P = 0.0169) genotypes or the XPA-mutant allele (OR = 3.56; 95% CI 1.53-8.25, P = 0.0012). These findings indicate that a complex interaction between host factors such as oxidative stress, antioxidant capacity and efficiency of multiple DNA repair pathways underlies the inter-individual variability in GC risk.

AB - Risk factors for gastric cancer (GC) include inter-individual variability in the inflammatory response to Helicobacter pylori infection, in the ability of detoxifying DNA reactive species and repairing DNA damage generated by oxidative stress and dietary carcinogens. To evaluate the association between polymorphic DNA repair genes and GC risk, a case-control study including 314 histologically confirmed GC patients and 548 healthy controls was conducted in a GC high-risk area in Tuscany, Italy. Polymorphic variants of base excision repair (APE1-D148E, XRCC1-R194W, XRCC1-R399Q and OGG1-S326C), nucleotide excision repair (XPC-PAT, XPA-23G>A, ERCC1-19007T>C and XPD-L751Q), recombination (XRCC3-T241M) and alkylation damage reversal (MGMT-L84F) were tested for their potential role in the development of GC by using logistic regression models. The same population was also characterised for GSTT1 and GSTM1 variant alleles to search for possible functional interactions between metabolic and DNA repair genotypes by two-way interactions using multivariate logistic models. No significant association between any single DNA repair genotype and GC risk was detected with a borderline association with the XPC-PAT homozygous genotype [odds ratio (OR) = 1.42; 95% confidence interval (CI) 0.94-2.17]. Gene-gene interaction analysis revealed combinations of unfavourable genotypes involving either multiple DNA repair polymorphisms or DNA repair and GST-specific genotypes. The combination of the XPC-PAT and the XPA variant alleles significantly increased GC risk (OR = 2.15; 95% CI 1.17-3.93, P = 0.0092). A significant interaction was also found between the APE1 wild-type genotype and either the single GSTT1 (OR = 4.90; 95% CI 2.38-10.11, P = 0.0079) or double GSTM1-GSTT1 null (OR = 7.84; 95% CI 3.19-19.22, P = 0.0169) genotypes or the XPA-mutant allele (OR = 3.56; 95% CI 1.53-8.25, P = 0.0012). These findings indicate that a complex interaction between host factors such as oxidative stress, antioxidant capacity and efficiency of multiple DNA repair pathways underlies the inter-individual variability in GC risk.

KW - DNA repair

KW - polymorphisms

KW - gastric cancer

KW - DNA repair

KW - polymorphisms

KW - gastric cancer

UR - https://iris.uniupo.it/handle/11579/223163

U2 - 10.1093/mutage/geq042

DO - 10.1093/mutage/geq042

M3 - Article

SN - 0267-8357

VL - 25

SP - 569

EP - 575

JO - Mutagenesis

JF - Mutagenesis

IS - 6

ER -

Polymorphic DNA repair and metabolic genes: a multigenic study on gastric cancer

Abstract

OSS delle Nazioni Unite

Keywords

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